4.8 Article

Structural basis for amino acid export by DMT superfamily transporter YddG

Journal

NATURE
Volume 534, Issue 7607, Pages 417-+

Publisher

NATURE PUBLISHING GROUP
DOI: 10.1038/nature17991

Keywords

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Funding

  1. Platform for Drug Discovery, Informatics and Structural Life Science by the Ministry of Education, Culture, Sports, Science and Technology (MEXT)
  2. JSPS KAKENHI [24227004, 25291011, 26711003]
  3. FIRST program
  4. Grants-in-Aid for Scientific Research [15K17882, 15J08129, 16H04710, 16H02420, 16H06294, 26711003, 26410190] Funding Source: KAKEN

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The drug/metabolite transporter (DMT) superfamily is a large group of membrane transporters ubiquitously found in eukaryotes, bacteria and archaea, and includes exporters for a remarkably wide range of substrates, such as toxic compounds and metabolites(1). YddG is a bacterial DMT protein that expels aromatic amino acids and exogenous toxic compounds, thereby contributing to cellular homeostasis(2,3). Here we present structural and functional analyses of YddG. Using liposome-based analyses, we show that Escherichia coli and Starkeya novella YddG export various amino acids. The crystal structure of S. novella YddG at 2.4 resolution reveals a new membrane transporter topology, with ten transmembrane segments in an outward-facing state. The overall structure is basket-shaped, with a large substrate-binding cavity at the centre of the molecule, and is composed of inverted structural repeats related by two-fold pseudosymmetry. On the basis of this intramolecular symmetry, we propose a structural model for the inward-facing state and a mechanism of the conformational change for substrate transport, which we confirmed by biochemical analyses. These findings provide a structural basis for the mechanism of transport of DMT superfamily proteins.

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